Renal Transplantation Clinical Trial
Official title:
Catalytic Antibodies to Predict Uninvasively Late Transplant Failure
Chronic Allograft Nephropathy (CAN), a major cause of late allograft failure, is characterized by a progressive decline in graft function correlating with tissue destruction. Recent data suggest that it may be possible to delay graft destruction if adequate management is initiated early (ie, at the stage of subclinical CAN). It is therefore essential to design new tests allowing physicians to predict transplant recipients prone to develop CAN
Superantibodies are multifunctional antibodies combining the classical antigen-binding
function with nonclassical biological activities, such as protease-like activity. In the
past few years the role of proteolytic SuperAntibody (pSAb) has been evidenced in many
biological processes in which their role may be either deleterious (autoimmune disease,
alloimmune response against) or beneficial (sepsis).
Nothing is known so far regarding the role of pSAb in the setting of solid organ
transplantation.
Preliminary data
The investigator has obtained preliminary results from a retrospective case control study
indicating that an elevated serine protease activity of circulating IgG (measured by the
hydrolysis of a synthetic fluorescent substrate:
Proline-Phenylalanine-Arginine-Methylcoumarinamide (PFR-MCA)), correlates with the absence
of CAN on protocol biopsy performed 2 years post-transplantation. Interestingly, low level
of proteolysis IgG, measured 3 months post-transplantation, were also predictive of CAN at 2
years down the lane.
Aim of the Research project:
The aim is to validate in a prospective study, the potential of pSAb as predictive marker
for CAN
100 recipients of a renal graft have to be enrolled and followed for 2 years.
The level of PFR-MCA hydrolysis by circulating Immunoglobulin G (IgG) will be measured
before the transplantation and every 3 months up to one year and every 6 months thereafter
until 2 year post-transplantation. The development of CAN will be assessed by estimated
glomerular filtration rate (Modification of the Diet in Renal Disease (MDRD) formula), the
proteinuria and the histological examination of the graft (screening biopsy at 3 months and
1 year will be analysed using a computerized color image analysis to quantify interstitial
fibrosis).
The capacity of the pSAb test to predict CAN will be validated and the sensibility and
specificity of this test will be calculated. The optimal cut-off value will be determined
from the Receiver Operating Characteristic (ROC) analysis. The accuracy of the test will be
evaluated in subgroups displaying various risk factors for CAN.
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Intervention Model: Single Group Assignment, Masking: Open Label
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